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Research ArticleBrain

[11C]Methionine PET, Histopathology, and Survival in Primary Brain Tumors and Recurrence

S. Ceyssens, K. Van Laere, T. de Groot, J. Goffin, G. Bormans and L. Mortelmans
American Journal of Neuroradiology August 2006, 27 (7) 1432-1437;
S. Ceyssens
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K. Van Laere
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T. de Groot
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J. Goffin
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G. Bormans
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L. Mortelmans
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Abstract

BACKGROUND AND PURPOSE: [11C]Methionine (MET) PET imaging is a sensitive technique for visualizing primary brain tumors and recurrence/progression after therapy. The aim of this study was to evaluate the relationship between the uptake of MET and histopathologic grading and to investigate the prognostic value of the tracer, in both settings.

METHODS: Cerebral uptake of MET was determined in 52 patients: in 26 patients for primary staging (group A) and 26 patients with suspected brain tumor recurrence/progression after therapy (group B). Semiquantitative methionine uptake indices (UI) defined by the tumor (maximum)-to-background ratio was correlated with tumor grade and final outcome.

RESULTS: Overall median survival was 34.9 months. MET showed pathologically increased uptake in 41 of 52 scans. Although a weak linear correlation between MET uptake and grading was observed (R = 0.38, P = .028), analysis of variance showed no significant differences in MET UI between tumor grades for either group A or B. Benign and grade I lesions showed significant difference in MET uptake in comparison with higher grade lesions (P = .006). Using Kaplan-Meier survival analysis, no thresholds could be found at which MET was predictive for survival. Proportional hazard regression showed that only WHO grading class (low versus high) was predictive of survival (P = .015).

CONCLUSION: Interindividual MET uptake variability does not allow noninvasive grading on an individual patient basis. Moreover, there is no significant prognostic value in studying maximal methionine UI in brain tumors. The clinical use of MET should therefore be primarily focused on questions such as detection of recurrence, biopsy guidance, and radiation therapy target volume delineation.

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American Journal of Neuroradiology: 27 (7)
American Journal of Neuroradiology
Vol. 27, Issue 7
August 2006
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S. Ceyssens, K. Van Laere, T. de Groot, J. Goffin, G. Bormans, L. Mortelmans
[11C]Methionine PET, Histopathology, and Survival in Primary Brain Tumors and Recurrence
American Journal of Neuroradiology Aug 2006, 27 (7) 1432-1437;

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[11C]Methionine PET, Histopathology, and Survival in Primary Brain Tumors and Recurrence
S. Ceyssens, K. Van Laere, T. de Groot, J. Goffin, G. Bormans, L. Mortelmans
American Journal of Neuroradiology Aug 2006, 27 (7) 1432-1437;
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Cited By...

  • Molecular imaging of 1p/19q deletion in oligodendroglial tumours with 11C-methionine positron emission tomography
  • Evaluation of the Biodistribution of 11C-Methionine in Children and Young Adults
  • Correlation of 18F-FLT Uptake with Tumor Grade and Ki-67 Immunohistochemistry in Patients with Newly Diagnosed and Recurrent Gliomas
  • 11C-Methionine PET for Grading and Prognostication in Gliomas: A Comparison Study with 18F-FDG PET and Contrast Enhancement on MRI
  • Multimodality Assessment of Brain Tumors and Tumor Recurrence
  • Value of 1H-magnetic resonance spectroscopy chemical shift imaging for detection of anaplastic foci in diffusely infiltrating gliomas with non-significant contrast-enhancement
  • Kinetics of 3'-Deoxy-3'-18F-Fluorothymidine During Treatment Monitoring of Recurrent High-Grade Glioma
  • Methyl-L-11C-Methionine PET as a Diagnostic Marker for Malignant Progression in Patients with Glioma
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